| Literature DB >> 34866326 |
Ranjana Maurya1, Anuj Tripathi1, Cyrille Y Botté2, T S Keshava Prasad3,4,5, Pushkar Sharma1, Manish Kumar1,3,6, Neelam Antil3,7,4, Yoshiki Yamaryo-Botté2, Praveen Kumar1, Priyanka Bansal1, Christian Doerig8.
Abstract
PfCDPK7 is an atypical member of the calcium-dependent protein kinase (CDPK) family and is crucial for the development of Plasmodium falciparum. However, the mechanisms whereby PfCDPK7 regulates parasite development remain unknown. Here, we perform quantitative phosphoproteomics and phospholipid analysis and find that PfCDPK7 promotes phosphatidylcholine (PC) synthesis by regulating two key enzymes involved in PC synthesis, phosphoethanolamine-N-methyltransferase (PMT) and ethanolamine kinase (EK). In the absence of PfCDPK7, both enzymes are hypophosphorylated and PMT is degraded. We further find that PfCDPK7 interacts with 4'-phosphorylated phosphoinositides (PIPs) generated by PI4-kinase. Inhibition of PI4K activity disrupts the vesicular localization PfCDPK7. P. falciparum PI4-kinase, PfPI4K is a prominent drug target and one of its inhibitors, MMV39048, has reached Phase I clinical trials. Using this inhibitor, we demonstrate that PfPI4K controls phospholipid biosynthesis and may act in part by regulating PfCDPK7 localization and activity. These studies not only unravel a signaling pathway involving PfPI4K/4'-PIPs and PfCDPK7 but also provide novel insights into the mechanism of action of a promising series of candidate anti-malarial drugs.Entities:
Keywords: CDPK; kinase; malaria; phospholipids; phosphoproteomics; signaling
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Year: 2021 PMID: 34866326 PMCID: PMC8811644 DOI: 10.15252/embr.202154022
Source DB: PubMed Journal: EMBO Rep ISSN: 1469-221X Impact factor: 8.807